Psychotropic drugs and liver disease: A critical review of pharmacokinetics and liver toxicity

doi:10.4292/wjgpt.v8.i1.26

Advanced Search

BPG is committed to discovery and dissemination of knowledge

Home / Archive / Volume 8, Issue 1

This Article

Academic Content and Language Evaluation of This Article

CrossCheck and Google Search of This Article

Academic Rules and Norms of This Article

Citation of this article

Corresponding Author of This Article

Research Domain of This Article

Article-Type of This Article

Open-Access Policy of This Article

Times Cited Counts in Google of This Article

Number of Hits and Downloads for This Article

Total Article Views (45618)

All Articles published online

The chart showing PDF series, WORD series, HTML series, Tables (1-5) series.

Item

Count

PDF

2330

WORD

538

HTML

39770

Tables (1-5)

340

Sum=42978

Publishing Process of This Article

The chart showing Browse series, Download series.

Item

Count

Browse

1251

Download

1389

Sum=2640

Feb 6, 2017 (publication date) through May 14, 2024

Times Cited of This Article

Times Cited (73)

Journal Information of This Article

Publication Name

World Journal of Gastrointestinal Pharmacology and Therapeutics

ISSN

2150-5349

Publisher of This Article

Baishideng Publishing Group Inc, 7041 Koll Center Parkway, Suite 160, Pleasanton, CA 94566, USA

Review

World J Gastrointest Pharmacol Ther. Feb 6, 2017; 8(1): 26-38
Published online Feb 6, 2017. doi: 10.4292/wjgpt.v8.i1.26

Table 1 Psychotropic drugs with extensive first-pass metabolism[10-16]

Tricyclic antidepressants - first-pass metabolism greater than 50% after oral administration

SNRI antidepressants - venlafaxine

SSRI antidepressants - sertraline

NRI antidepressants - bupropion

Typical antipsychotics - chloropromazine

Atypical antipsychotics - olanzapine (40%), quetiapine

SSRI: Selective serotonin reuptake inhibitors; SNRI: Serotonin and norepinephrine reuptake inhibitors; NRI: Norepinephrine reuptake inhibitors.

Table 2 Antidepressants and liver toxicity

	Epidemiology	Type of lesion	Mechanism
Tricyclic antidepressants
Imipramine	ALT transient elevation-20%[45] Cholestatic jaundice: 0.5%-1%[2] DILI: 4/100000 patient-years[2,46] Fatal/Trxp DILI: 1[47]	Hepatocellular, cholestatic	Immuno-allergic
Amitriptiline	ALT transient elevation-10%[45] Abnormal LFT: 3%[48] Fatal/Trxp DILI: 1[39]	Hepatocellular, cholestatic	Immuno-allergic
Clomipramine	Severe DILI: 2 reports[42,49]	Hepatocellular	Immuno-allergic
MAO inibitors
Moclobemide	Abnormal LFT: 3%[50] Fatal DILI: 1[51]	Hepatocellular, cholestatic	Immuno-allergic
Serotonin-norepinephrine reuptake inhibitors
Venlafaxine	ALT > 3ULN: 0.4%[52] Severe DILI: 6[53-56] Fatal DILI/Trxp: 1[57]	Hepatocellular, cholestatic	Immuno-allergic, metabolic
Duloxetine	ALT > 3ULN: 1.1%[58] ALT > 5ULN: 0.6%[59] DILI: 26.2/100000 patient-years[60,61] Severe DILI-7[5] Fatal/Trxp DILI: 13[60]	Hepatocellular, cholestatic, mixed	Immuno-allergic, metabolic
Serotonin-reuptake inhibitors
Sertraline	ALT > 3ULN: 0.5%-1.3%[46] DILI: 1.28/100000 patient-years[46] Severe DILI: 4[62-65] Fatal/Trxp DILI: 2[66,67]	Hepatocellular, cholestatic, mixed	Immuno-allergic, metabolic
Paroxetine	ALT > 3ULN: 1%[46] Severe DILI: 4[68-71]	Hepatocellular, cholestatic, chronic hepatitis	Metabolic
Fluoxetine	ALT > 3ULN: 0.5%[46] Severe DILI: 6[72-77]	Hepatocellular, cholestatic, chronic hepatitis	Metabolic
Fluvoxamine	Unknown[38] DILI: 3[78-80]	Hepatocellular	Metabolic
Citalopram, escitalopram	No difference in LFT vs placebo[81,82]	?	?
Other antidepressants
Nefazodone	DILI: 28.96/10000 patient-years[38] Severe DILI-35[83] Fatal-20[83]	Hepatocellular, cholestatic, mixed	Metabolic
Trazodone	ALT > 3 unknown[38] Severe DILI-7[84] Fatal/Trxp DILI-2[57,85]	Hepatocellular, cholestatic	Immuno-allergic
Bupropion	ALT > 3ULN: 0.1%-1%[86] Severe DILI: 3[86-88] Fatal/Trxp DILI: 2[89,90]	?	?
Agomelatine	ALT > 3ULN: 1.4% (25 mg/d) ALT > 3ULN: 2.5% (50 mg/d)[6,91] Severe DILI: 6 reports[92,93] Fatal/Trxp DILI: 1[94]	Hepatocellular
Mirtazapine	ALT > 3ULN: 2%[95] Severe DILI 2: reports[96]

DILI: Drug-induced liver injury; ALT: Alanine aminotransferase; LFT: Liver function tests; ULN: Upper normal limit.

Table 3 Antipsychotics and liver toxicity

	Epidemiology	Type of lesion	Mechanism
Typical
Cloropromazine	Jaundice: 0.16%-0.3%[99] Severe DILI: > 350[100,101,115-124] Fatal Injury: 8[102-109]	Cholestatic	Immuno-allergic
Haloperidol	ALT > 3ULN: 2%[110] Severe DILI: 1[111]	Cholestatic	Immuno-allergic
Atypical
Clozapine	ALT > 3ULN: 15%[125] Severe DILI: 16[126-140] Fatal Injury: 2[141,142]	Hepatocellular Cholestatic Chronic esteatosis	Immuno-allergic Chronic estatosis
Olanzapine	ALT > 3ULN: 6%[143] Severe DILI: 7[139,144-149]	Hepatocellular Cholestatic Chronic esteatosis	Immuno-allergic, Chronic estatosis
Risperidone	ALT > 3ULN: 3%[150] Severe DILI: 13[150-162]	Hepatocellular Cholestatic Chronic esteatosis	Immuno-allergic Chronic estatosis
Quetiapine	ALT > 3ULN: 0%[143] Severe DILI: 3[151,163,164] Fatal injury: 2[165,166]	?	?
Ziprasidone	Not reported Severe DILI: 1[167]	?	?
Aripiprazole	Not reported
Amissulpride	Not reported

DILI: Drug-induced liver injury; ALT: Alanine aminotransferase; ULN: Upper normal limit.

Table 4 Mood stabilizers and benzodiazepines and liver toxicity

	Epidemiology	Type of lesion	Mechanism
Antiepileptics
Carbamazepine	Transient ALT, AST, GGT elevations: 61% patients 1%-22%[3] DILI: 1%[170]	Hepatocellular, cholestatic	++Hypersensitivity -- Metabolic
Valproate	Transient ALT, AST elevations: 10%-15% patients[170] Hyperrubillirubinemia-44%[170] DILI: 3%-44%[173] Fatal DILI: 0.02% (0.2% children < 2a)[1]	Hepatocellular	Metabolic (Toxic metabolites through w-oxidation) Statosis
Lamotrigine	Transient ALT, AST elevations < 1% Rare hepatotoxicity[170] (4 severe DILI)[174]	Hepatocellular	Metabolic
Topiramate	Transient ALT, AST elevations < 1%[1] Rare hepatotoxicity (2 severe DILI)[174]	Hepatocellular	Metabolic
Gabapentine; pregabaline	Rare hepatotoxicity[1]	?	?
Benzodiazepines
Chlordiazepoxide, diazepam, flurazepam	Rare hepatotoxicity[171,172]	Cholestatic	Hypersensitivity
Litium
	Very rare hepatotoxicity[1]	?	?

DILI: Drug-induced liver injury; ALT: Alanine aminotransferase; AST: Aspartate aminotransferase; GGT: Gamma-glutamyl transferase.

Table 5 Pharmacokinetic changes caused by end-stage liver disease: Psychotropic drugs that require special attention

Avoid drugs with extensive first-pass metabolism	Avoid Tricyclic Antidepressants (first-pass metabolism 50%), venlafaxine, sertraline, bupropion, chlorpromazine, quetiapine
Avoid highly protein bound drugs	Avoid most psychotropic drugs (specially fluoxetine, aripiprazole and benzodiazepines). Except: Venlafaxine, lithium, topiramate, a gabapentin, a pregabalin, memantine
Avoid drugs depending on phase I hepatic metabolic reactions	Preferable: Lithium, gabapentin, topiramate, amisulpride (depending mainly on renal excretion) and some benzodiazepines (oxazepam, temazepam, lorazepam) that depend on phase II reaction or glucuronidation, which is preserved in cirrhosis

Citation: Telles-Correia D, Barbosa A, Cortez-Pinto H, Campos C, Rocha NBF, Machado S. Psychotropic drugs and liver disease: A critical review of pharmacokinetics and liver toxicity. World J Gastrointest Pharmacol Ther 2017; 8(1): 26-38
URL: https://www.wjgnet.com/2150-5349/full/v8/i1/26.htm
DOI: https://dx.doi.org/10.4292/wjgpt.v8.i1.26